Overactive Bladder Clinical Trial
Official title:
A Double-Blind, Randomized Study of the Safety and Efficacy of OnabotulinumtoxinA (OnaBoNT-A) Versus Oral Oxybutynin in Spinal Cord Injured Patients With Neurogenic Detrusor Overactivity (Protocol Number 11-09-10-04)
Overactive bladder is a condition associated with symptoms of feeling the urge to urinate,
urinating often, and may or may not be accompanied by leakage of urine. A patient who has a
spinal cord injury (SCI) often suffers from an overactive bladder which often leads to
urinary incontinence (UI - an unwanted leakage of urine).
OnaBoNT-A bladder injections have been studied in clinical research trials. The results have
shown an improvement in urinary symptoms by reducing how often urine leakage occurs and by
increasing the amount of urine the bladder can hold.
This purpose of this clinical trial is to see if onaBoNT-A is safe and effective when
injected into the bladder for the treatment of UI and if it works better than a drug that is
taken by mouth. A second purpose of the study is to perform research tests on the urine
samples provided by the volunteers. Urine presents a rich source of information for bladder
diseases and the biomarkers (the chemical make-up of the urine cells) will be examined to
learn if there are yet undiscovered reasons for urinary diseases. These tests would be very
beneficial because the results would lead to better treatment of the urinary diseases.
Volunteers will be randomized to either: ARM 1: onaBoNT-A 200 U bladder injection and
placebo oral capsule daily or ARM 2: Placebo bladder injection (saline) and oxybutynin ER
10mg capsule twice a day.
The treatments are onaBoNT-A bladder injection and a placebo oral capsule once a day or
placebo bladder injection and oxybutynin ER (like Ditropan) capsule twice a day. Placebo
contains no active medicine. Participation in this study will be about 6-7 months and
involve 5 visits to the clinic. The risks of bladder onaBoNT-A
Current treatment of neurogenic bladder dysfunction (NGB) is limited by the suboptimal
results achieved using standard antimuscarinic agents. A prominent role for the actions of
alternative transmitters/growth factors in peripheral micturition pathways is emerging from
the growing number of pharmacologic and localization studies in humans. For example,
recently published data demonstrates a significant increased expression of Nerve Growth
Factor and chemokine/cytokine levels in patients with detrusor overactivity and NGB.
Treatment with onabotulinumtoxinA (onaBoNT-A) not only was shown to reduce detrusor
overactivity and improve urinary symptoms but also significantly reduced tissue and urine
levels of factors such as NGF. Up to this point, no study has directly compared the effects
of front-line therapy of antimuscarinic agents versus onaBoNT-A on urinary symptoms in
patients with NGB resulting from spinal cord injury (SCI). In addition, no investigation has
examined the effects that antimuscarinic agents or onaBoNT-A have on urinary levels of NGF
and chemokines/cytokines, whether changes in urinary levels predict a clinical response or a
return in symptoms, and if changes in urinary levels predate changes in clinical response.
Access to selective and reliable urine testing of NGF and chemokines/cytokines provides the
unique opportunity to assess the impact that modulating these agents has on bladder
function. The main purpose of this proposal is to incorporate novel urine biomarker testing
into existing clinical methodologies in order to: 1) evaluate the safety and efficacy of 200
U onaBoNT-A injected into the detrusor versus oral oxybutynin for the treatment of urinary
incontinence (UI) caused by neurogenic detrusor overactivity (NDO) in spinal cord injured
patients and 2) to determine the potential role of urine biomarkers in guiding the process
of patient selection and identify surrogate predictors of treatment outcomes.
This will be a double-blind, randomized, placebo-controlled, parallel-group study to assess
the safety and efficacy of onaBoNT-A or 10 mg twice a day of oral oxybutynin hydrocholoride
in spinal cord injured patients diagnosed with neurogenic detrusor overactivity.
Volunteers will include both males and females with spinal cord injuries who are 18 to 80
years of age.
Volunteers will be randomized using a blocked randomization approach to either:
ARM 1: onaBoNT-A 200 U bladder injection and placebo oral capsule daily or
ARM 2: Placebo bladder injection (saline) and oxybutynin ER 10mg capsule twice a day.
Subjects will be randomized into one of the two treatment arms, using a block size of 4. The
order in which the treatments are assigned in each block is randomized and this process is
repeated for consecutive blocks of subjects until all subjects are randomized. This process
ensures that after every fourth randomized subject, the number of subjects in each treatment
group is equal.
There will be five study visits over approximately 6-7 months.
The significance of these experiments begins with the fact that our proposed intervention is
the first randomized clinical trial comparing the effects of onaBoNT-A (onabotulinumtoxinA)
bladder injection versus anticholinergic medication for detrusor hyperreflexia (DH). In
addition, this is the first study profiling urine levels of the signaling protein nerve
growth factor (NGF) and chemokines/cytokines as possible bio-markers of bladder overactivity
in patients with neurogenic detrusor overactivity. Finally, this is the only study to date
comparing the effects that onaBoNT-A or anticholinergic medications have on urine NGF and
chemokine/cytokine levels. If our hypotheses prove to be correct, the significance to
treating patients with spinal cord injury with botulinum toxin A will be less incontinence,
the requirement of lower doses or avoidance of anticholinergic medication and its associated
side effects, and the ability to prevent the complications of DH/DESD (Detrusor-External
Sphincter Dyssynergia) including urinary tract infections, decubiti, and impairment of
quality of life. Although this study as written is of moderate length (i.e. total 4 years),
we hope that by finding significant results, we will be able to capture a longitudinal
history of this population by extending follow-up to a longer duration (i.e. over 10 years).
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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